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CHROMOSOME STRUCTURE AND DYNAMICS

Recql5 and Blm RecQ DNA Helicases Have Nonredundant Roles in Suppressing Crossovers

Yiduo Hu, Xincheng Lu, Ellen Barnes, Min Yan, Hua Lou, Guangbin Luo
Yiduo Hu
1Department of Genetics
2Case Comprehensive Cancer Center, University Hospitals of Cleveland, Cleveland, Ohio
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Xincheng Lu
1Department of Genetics
2Case Comprehensive Cancer Center, University Hospitals of Cleveland, Cleveland, Ohio
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Ellen Barnes
1Department of Genetics
2Case Comprehensive Cancer Center, University Hospitals of Cleveland, Cleveland, Ohio
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Min Yan
1Department of Genetics
3Department of Molecular Biology and Microbiology, Case Western Reserve University
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Hua Lou
1Department of Genetics
2Case Comprehensive Cancer Center, University Hospitals of Cleveland, Cleveland, Ohio
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Guangbin Luo
1Department of Genetics
2Case Comprehensive Cancer Center, University Hospitals of Cleveland, Cleveland, Ohio
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  • For correspondence: GXL35@case.edu
DOI: 10.1128/MCB.25.9.3431-3442.2005
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ABSTRACT

In eukaryotes, crossovers in mitotic cells can have deleterious consequences and therefore must be suppressed. Mutations in BLM give rise to Bloom syndrome, a disease that is characterized by an elevated rate of crossovers and increased cancer susceptibility. However, simple eukaryotes such as Saccharomyces cerevisiae have multiple pathways for suppressing crossovers, suggesting that mammals also have multiple pathways for controlling crossovers in their mitotic cells. We show here that in mouse embryonic stem (ES) cells, mutations in either the Bloom syndrome homologue (Blm) or the Recql5 genes result in a significant increase in the frequency of sister chromatid exchange (SCE), whereas deleting both Blm and Recql5 lead to an even higher frequency of SCE. These data indicate that Blm and Recql5 have nonredundant roles in suppressing crossovers in mouse ES cells. Furthermore, we show that mouse embryonic fibroblasts derived from Recql5 knockout mice also exhibit a significantly increased frequency of SCE compared with the corresponding wild-type control. Thus, this study identifies a previously unknown Recql5-dependent, Blm-independent pathway for suppressing crossovers during mitosis in mice.

  • Copyright © 2005 American Society for Microbiology
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Recql5 and Blm RecQ DNA Helicases Have Nonredundant Roles in Suppressing Crossovers
Yiduo Hu, Xincheng Lu, Ellen Barnes, Min Yan, Hua Lou, Guangbin Luo
Molecular and Cellular Biology Apr 2005, 25 (9) 3431-3442; DOI: 10.1128/MCB.25.9.3431-3442.2005

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Recql5 and Blm RecQ DNA Helicases Have Nonredundant Roles in Suppressing Crossovers
Yiduo Hu, Xincheng Lu, Ellen Barnes, Min Yan, Hua Lou, Guangbin Luo
Molecular and Cellular Biology Apr 2005, 25 (9) 3431-3442; DOI: 10.1128/MCB.25.9.3431-3442.2005
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KEYWORDS

Adenosine Triphosphatases
Bloom Syndrome
Crossing Over, Genetic
DNA Helicases
Sister Chromatid Exchange

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